INHIBITION OF GLUTATHIONE-RELATED ENZYMES AND CYTOTOXICITY OF ETHACRYNIC-ACID AND CYCLOSPORINE

被引:17
|
作者
HOFFMAN, DW
WIEBKIN, P
RYBAK, LP
机构
[1] SO ILLINOIS UNIV,SCH MED,DEPT SURG ENT,SPRINGFIELD,IL 62708
[2] SO ILLINOIS UNIV,SCH MED,DEPT PHARMACOL,SPRINGFIELD,IL 62708
关键词
CANCER; CHEMOTHERAPY; ANTINEOPLASTIC AGENT; GLUTATHIONE S-TRANSFERASE; GLUTATHIONE REDUCTASE; DIURETIC;
D O I
10.1016/0006-2952(94)00474-Z
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Glutathione (GSH) is an endogenous thiol that detoxifies active oxygen and reactive species formed during intermediary metabolism and drug detoxification. Compounds with a range of potential toxicities were tested for their abilities to affect GSH reductase and GSH S-transferase activities, which are each components of the two principal detoxification pathways in which GSH participates. A high performance liquid chromatographic method for determining oxidized and reduced GSH was modified to assay GSH reductase activity. With this method it was possible to demonstrate that ethacrynic acid, which inhibits GSH S-transferase, also inhibits the activity of GSH reductase. Inhibition of GSH reductase by ethacrynic acid was similar to that seen with carmustine (BCNU). GSH reductase activity was not affected by cis- or transplatin, buthionine sulfoximine, other loop diuretics, cyclosporine A or aminoglycosides. Cyclosporine inhibited GSH S-transferase at 50 mu M and higher concentrations. These results support a role for GSH-mediated detoxification mechanisms in ethacrynic acid- and cyclosporine-associated cytotoxicity, which may mediate their toxicities and their potential as adjunctive agents in antineoplastic therapy. A better understanding of the mechanism of their toxicity can greatly extend the clinical usefulness of these agents, as this toxicity is the basis of both their therapeutic and antitherapeutic actions.
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页码:411 / 415
页数:5
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